MCADD (Medium-Chain Acyl-CoA Dehydrogenase Deficiency)
Guidance on diagnosing and managing children with MCADD
Medium-chain acyl-CoA dehydrogenase deficiency (MCADD) is a type of fatty acid oxidation disorder caused by a defect in the catabolism of medium-chain fatty acids. Fatty acid B-oxidation fuels hepatic ketogenesis, a major energy source after glycogen stores have been depleted. Impaired MCAD activity results in hypoketotic hypoglycemia during prolonged fasting or increased energy demands (e.g., acute illness or fever). Individuals with MCADD are usually diagnosed through newborn screening or after showing symptoms, which can occur at any age.
Key Points
Response to a positive newborn screen for MCADD
If notified of a positive newborn test result for MCADD, the medical
home should collaborate with a metabolic geneticist who will help verify the test
result and follow through with appropriate care and education for the patient and
the family. Medium-Chain Acyl-CoA Dehydrogenase Deficiency (MCADD) details initial
steps for confirming the diagnosis and immediate management.
Acute attacks can progress rapidly
Acute decompensation is more common during acute illness, fasting, or
other times of metabolic stress. Management revolves around fasting avoidance and
prompt treatment of acute episodes with intravenous (IV) glucose. [Feillet: 2012]
[Potter: 2012] If untreated, acute attacks of hypoglycemia
can rapidly progress to seizures, coma, and sudden death.
Atypical ketones are found in some individuals
Although nonketotic hypoglycemia is a hallmark presentation, some
affected individuals can generate some ketones.
Avoid alcohol consumption
Adolescents and adults with MCADD should be counseled about the
possible risks of excessive consumption of alcohol, which may include
encephalopathy, rhabdomyolysis, and cardiac failure. [Lang: 2009]
Emergency treatment letter needed
All families who have a child with MCADD should have an emergency
treatment letter that can be presented at the emergency room in case of illness. A
medical alert bracelet or necklace also can be worn to let providers know that the
child has MCADD, but it is not a substitution for the emergency letter. See Sample Letter for Emergency Care for the Child with MCADD (Medical Home Portal) ( 14 KB).
Management during an acute illness
Children with MCADD who are ill require early evaluation and
intervention. During an acute illness, any form of tolerable caloric intake is
necessary (e.g., juice, Gatorade, and Powerade). If unable to tolerate oral intake,
dextrose-containing IV fluids should be administered to maintain normoglycemia.
Occasionally, uncooked cornstarch (1-1½ g/kg) may be recommended by a metabolic
provider as a preventative measure for infants and young children. Levocarnitine (50
mg/kg/day) supplementation may also be recommended if experiencing a secondary
deficiency.
Home glucose monitoring may be unreliable
Hypoglycemia occurs after the onset of clinical symptoms and is an
unreliable marker for early decompensation or encephalopathy. Therefore, families
should speak with their metabolic provider about the usefulness of home glucose
monitoring for them. [Leonard: 2009]
Fasting at any age can lead to acute attacks
Although fasting tolerance improves with age, prolonged fasting in an
affected individual can lead to coma and death at any age. Patients should be
counseled to remain hydrated and consume additional calories during prolonged
physical activity.
Diagnosis
Presentations
Affected individuals may be asymptomatic until placed under the right amount of metabolic stress. The clinical presentation is indistinguishable from other hypoglycemia causes, including clamminess, irritability, lethargy, and vomiting. They may experience intermittent symptoms after periods of fasting or intercurrent illnesses. Less often, liver disease and hepatomegaly may be presenting features.
Diagnostic Criteria and Classifications
- Positive findings on expanded newborn screening
- Nonketotic hypoglycemia
- Elevations of C8, C6, C10, C10:1 acylcarnitines
- Elevations of urinary dicarboxylic acids, hexanoylglycine, suberylglycine, and cis-4-decenoic acid
- DNA testing identifying the common A985G variant and/or other pathogenic variants in the ACADM gene
Screening & Diagnostic Testing
Laboratory Testing
MCADD is included in all US states’ expanded newborn screening panes. With expanded newborn screening, the diagnosis is suspected when elevations of C8, C6, and C10:1 are seen on tandem mass spectrometry. Follow-up confirmatory testing typically includes:
- Plasma acylcarnitine analysis with elevations of C8, C6, C10, C10:1
- Urine organic acids with elevations of hexanoylglycine, octanoylglycine, decanoylglycine; may also see elevated dicarboxylic acids adipic, suberic, sebacic, and dodecanedioic
- Urine acylglycine with elevations of n-hexanoylglycine, 3-phenylpropionylglycine, and suberylglycine
Genetic Testing
DNA testing of the ACADM gene should be done to confirm the diagnosis. Though the A985G variant is most common, sequencing of the entire gene is recommended.
Analysis of fatty acid beta-oxidation in cultured fibroblasts or MCAD enzyme activity in leukocytes, fibroblasts, liver, heart, or skeletal muscle can be used to confirm a diagnosis that remains in question either due to the absence of ACADM variants or variants of uncertain significance. [Alcaide: 2022]
Testing for Family Members
If a patient is confirmed to have MCADD, then it is assumed that both parents are carriers. Testing of asymptomatic siblings who have passed newborn screening in the US is not necessary. However, the family should be counseled regarding the recurrence risk for future children who can be tested at the time of birth rather than waiting for the newborn screen to return.
Prenatal diagnosis by either molecular genetic or biochemical testing is possible; however, this must be done by either amniocentesis or chorionic villus sampling (CVS). It is felt that there is no advantage to prenatal testing if prompt postnatal testing by measurement of plasma acylcarnitines and urine acylglycines is obtained in at-risk pregnancies. [Onunaku: 2005]
Pregnant women with MCADD are at increased risk of experiencing pregnancy complications such as hemolysis, elevated liver enzymes, low platelets (HELLP) syndrome, and acute fatty liver of pregnancy (AFLP). [Browning: 2006] [Santos: 2007]
Genetics & Inheritance
Parents of a child with MCADD are counseled that they have a 25% chance of having an affected baby, a 50% chance of having a baby who is a carrier, and a 25% chance of having a baby who is neither affected nor a carrier. Unaffected siblings have a 67% chance of being carriers of the disorder. All of the children of an affected individual will be, at the least, carriers. The probability of having an affected child depends on the carrier status of the other parent.
Prevalence
Differential Diagnosis
Important clinical features that might help differentiate MCADD from the other fatty acid oxidation disorders (e.g., very long-chain acyl-CoA dehydrogenase deficiency, long-chain 3-hydroxylacyl-CoA dehydrogenase deficiency, carnitine palmitoyl transferase I/II deficiencies, carnitine transporter defect, and carnitine translocase deficiency) include the absence of cardiomyopathy and/or rhabdomyolysis, which are common among these other conditions. The biochemical pattern of MCADD is very specific, though, and can be differentiated from other fatty acid oxidation disorders.
Ketogenesis defects
The ketogenesis defects often present within the first few days of life. The pattern of presentation in later childhood and some presenting symptoms, such as vomiting, decreased sensorium, and hepatomegaly, may be very similar to MCADD. Although hypoketotic hypoglycemia and sometimes hyperammonemia are biochemical features, severe ketoacidosis is the rule.
Organic acidurias
Most organic acidurias present with hyperketotic hypoglycemia rather than hypoketotic hypoglycemia.
Carbohydrate metabolism defects
Carbohydrate metabolism defects may present with hypoglycemia, significant lactic acidosis, +/- ketosis, and hepatomegaly. Acylcarnitine profile and urine organic acid profile will help differentiate these disorders from MCADD.
Co-occuring Conditions
Prognosis
Prognosis is excellent when treatment for MCADD is initiated before decompensation, including fasting avoidance and proper management during intercurrent illnesses. Prior to identification by expanded newborn screening, up to 29% of undiagnosed patients died during the first decompensation. [Lang: 2009] Those who survive an acute episode of decompensation may develop mild to severe sequelae
Treatment & Management
Endocrine/Metabolism
With prolonged fasting, lipolysis and hepatic fatty acid oxidation become activated. Plasma levels of free fatty acids rise, but ketones remain inappropriately low. Patients then become hypoglycemic with progressive lethargy, confusion, nausea, and vomiting. Hepatomegaly is sometimes noted. Without rapid intervention with IV glucose, hypoglycemia can rapidly progress to seizures, coma, and sudden death.
The following general guidelines are recommended, though they should be taken on a case-by-case basis and not include situations in which there is an extra metabolic stressor:
- Infants should be fed frequently; fasting should not exceed 3 to 4 hours
- Between 6 months and 1 year of age, fasting should not exceed 8 hours
- Between 1 to 2 years of age, fasting should not exceed 10 hours
- For individuals older than 2 years, fasting should not exceed 12 hours
Treatment of ill patients with MCADD involves:
- IV fluid therapy, preferably with D10 (and electrolytes per clinical discretion) at 1.5-2 x maintenance, should be given to maintain normoglycemia.
- If a patient becomes ill, prompt administration of IV glucose is mandatory. Delay in treatment may lead to sudden death or permanent neurologic sequelae. Under no circumstances should the administration of IV glucose be delayed.
- Oral glucose gel or other forms of simple sugars that can be absorbed by the mucus membranes may be kept available for families and used in emergency situations as a temporary solution while seeking medical care.
The use of carnitine is controversial but indicated when there is a secondary carnitine deficiency. [Lee: 2005] If supplementation with carnitine is necessary, it should be initiated under the guidance of the metabolic specialist. It had been recommended that the dose of L-carnitine be 50-100 mg/kg/day.
Nutrition/Growth/Bone
Learning/Education/Schools
Services & Referrals
Biochemical Genetics (Metabolics)
(see NM providers
[1])
Refer to a metabolic geneticist who, along with a metabolic
nutritionist, will educate the family about the disorder and its treatment. If the
diagnosis has not been made but is suspected, refer for testing. Periodic visits are
important to support families, monitor for problems, and provide needed education.
Refer if supplementation with carnitine is being considered. Consult for management
of diet and if the child becomes ill.
Nutrition, Metabolic
(see NM providers
[11])
The
nutritionist will play a critical role in formulating a healthy diet with the
necessary fats, carbohydrates, proteins, vitamins, minerals, and cofactors to allow
for proper growth and development.
Genetic Testing and Counseling
(see NM providers
[5])
Refer for assistance with genetic testing, interpretation of
results, and to discuss inheritance patterns, recurrence risks, and reproductive
options for the individual with MCADD and their family.
Pediatric Neurology
(see NM providers
[5])
Refer if
indicated by clinical presentation, especially if seizures are part of the initial
presentation or persistent.
Developmental - Behavioral Pediatrics
(see NM providers
[2])
Referral should be made if there is concern about sequelae after an
acute presentation or concern about specific developmental deficits.
ICD-10 Coding
E71.311, Medium-chain acyl-CoA dehydrogenase deficiency
ICD-10 for Medium-Chain Acyl-CoA Dehydrogenase Deficiency (icd10data.com) provides further coding details.
Resources
Information & Support
Related Portal Content
Medium-Chain Acyl-CoA Dehydrogenase Deficiency (MCADD)
Immediate response to a positive newborn test result.
Developmental Screening
Screening tools and guidance on response to a positive screen.
Formulas andFormulas for Metabolic Conditions ( 138 KB)General guidance and name brads
of formula.
Fatty Acid Oxidation Disorders (FAQ)
Answers to questions parent may frequently ask about their child
with MCADD's care.
For Professionals
MCADD (OMIM)
Information about clinical features, diagnosis, management, and molecular and population genetics; Online Mendelian Inheritance
in Man, authored and edited at the McKusick-Nathans Institute of Genetic Medicine, Johns Hopkins University School of Medicine
Medium-Chain Acyl-Coenzyme A Dehydrogenase Deficiency (GeneReviews)
Excellent review of MCADD that includes a clinical description, differential diagnoses, management information, and molecular
genetic information; sponsored by the U.S. National Library of Medicine.
Guidelines for MCADD (Genetic Metabolic Dietitians International)
Extensive clinical information about nutrition therapy for MCADD. Topics include background, signs and symptoms, laboratory
findings, biochemical basis of MCADD, chronic and acute management, monitoring, and special circumstances; edited by Dianne
M. Frazier, PhD, MPH, RD.
For Parents and Patients
Fatty Oxidation Disorders (FOD) Family Support Group
Information for families about fatty acid oxidation disorders, support groups, coping, finances, and links to other sites.
MCADD - Information for Parents (STAR-G)
A fact sheet, written by a genetic counselor and reviewed by metabolic and genetic specialists, for families who have received
an initial diagnosis of this newborn disorder; Screening, Technology and Research in Genetics.
Medium-chain acyl-CoA dehydrogenase deficiency (MedlinePlus)
Information for families that includes description, frequency, causes, inheritance, other names, and additional resources;
from the National Library of Medicine.
MCADD: A Guide for Parents (PacNoRGG) ( 618 KB)
Eight-page guide that includes an overview, social concerns, sample treatment plan, glossary, regional resources, and references;
sponsored by the Pacific Northwest Regional Genetics Group.
MCADD: A Guide for Parents (PacNoRGG) (Spanish) ( 202 KB)
Spanish translation of an 8-page guide that includes an overview, social concerns, sample treatment plan, glossary, regional
resources, and references; sponsored by the Pacific Northwest Regional Genetics Group.
Tools
Medium Chain Acyl-CoA Dehydrogenase Deficiency (MCADD) (NECMP) ( 17 KB)
Guideline for clinicians treating the sick infant or child who has MCADD; developed under the direction of Dr. Harvey Levy,
Senior Associate in Medicine/Genetics at Children’s Hospital Boston, and Professor of Pediatrics at Harvard Medical School,
for the New England Consortium of Metabolic Programs. Click pdf to view the complete protocol.
Sample Letter for Emergency Care for the Child with MCADD (Medical Home Portal) ( 14 KB)
A sample letter with emergency treatment details that can be provided to families who have a child with MCADD.
Confirmatory Algorithm for MCAD Deficiency ( 170 KB)
Resource for clinicians to help confirm diagnosis; American College of Medical Genetics.
Services for Patients & Families in New Mexico (NM)
Service Categories | # of providers* in: | NM | NW | Other states (3) (show) | | NV | RI | UT |
---|---|---|---|---|---|---|---|---|
Biochemical Genetics (Metabolics) | 1 | 1 | 2 | 3 | 2 | |||
Developmental - Behavioral Pediatrics | 2 | 1 | 3 | 12 | 9 | |||
Genetic Testing and Counseling | 5 | 5 | 11 | 7 | 10 | |||
Nutrition, Metabolic | 11 | 11 | 13 | 13 | 11 | |||
Pediatric Neurology | 5 | 5 | 18 | 8 |
For services not listed above, browse our Services categories or search our database.
* number of provider listings may vary by how states categorize services, whether providers are listed by organization or individual, how services are organized in the state, and other factors; Nationwide (NW) providers are generally limited to web-based services, provider locator services, and organizations that serve children from across the nation.
Studies
MCADD (ClinicalTrials.gov)
Studies looking at better understanding, diagnosing, and treating this condition; from the National Library of Medicine.
Helpful Articles
Gartner V, McGuire PJ, Lee PR.
Child Neurology: medium-chain acyl-coenzyme A dehydrogenase deficiency.
Neurology.
2015;85(4):e37-40.
PubMed abstract / Full Text
Gramer G, Haege G, Fang-Hoffmann J, Hoffmann GF, Bartram CR, Hinderhofer K, Burgard P, Lindner M.
Medium-Chain Acyl-CoA Dehydrogenase Deficiency: Evaluation of Genotype-Phenotype Correlation in Patients Detected by Newborn
Screening.
JIMD Rep.
2015;23:101-12.
PubMed abstract / Full Text
Rice GM, Steiner RD.
Inborn Errors of Metabolism (Metabolic Disorders).
Pediatr Rev.
2016;37(1):3-15; quiz 16-7, 47.
PubMed abstract
Schatz UA, Ensenauer R.
The clinical manifestation of MCAD deficiency: challenges towards adulthood in the screened population.
J Inherit Metab Dis.
2010.
PubMed abstract
Feillet F, Ogier H, Cheillan D, Aquaviva C, Labarthe F, Baruteau J, Chabrol B, de Lonlay P, Valayanopoulos V, Garnotel R,
Dobbelaere D, Briand G, Jeannesson E, Vassault A, Vianey-Saban C.
[Medium-chain acyl-CoA-dehydrogenase (MCAD) deficiency: French consensus for neonatal screening, diagnosis, and management].
Arch Pediatr.
2012;19(2):184-93.
PubMed abstract
Authors & Reviewers
Author: | Brian J. Shayota, MD, MPH |
2016: update: Laurie Smith, MD, Ph.D.SA; Natario Couser, MD, MSR |
2010: update: Laurie Smith, MD, Ph.D.A |
2008: first version: Holly WelshCA |
Page Bibliography
Alcaide P, Ferrer-López I, Gutierrez L, Leal F, Martín-Hernández E, Quijada-Fraile P, Bellusci M, Moráis A, Pedrón-Giner C,
Rausell D, Correcher P, Unceta M, Stanescu S, Ugarte M, Ruiz-Sala P, Pérez B.
Lymphocyte Medium-Chain Acyl-CoA Dehydrogenase Activity and Its Potential as a Diagnostic Confirmation Tool in Newborn Screening
Cases.
J Clin Med.
2022;11(10).
PubMed abstract / Full Text
Andresen BS, Bross P, Udvari S, Kirk J, Gray G, Kmoch S, Chamoles N, Knudsen I, Winter V, Wilcken B, Yokota I, Hart K, Packman
S, Harpey JP, Saudubray JM, Hale DE, Bolund L, Kølvraa S, Gregersen N.
The molecular basis of medium-chain acyl-CoA dehydrogenase (MCAD) deficiency in compound heterozygous patients: is there correlation
between genotype and phenotype?.
Hum Mol Genet.
1997;6(5):695-707.
PubMed abstract
Arnold GL, Saavedra-Matiz CA, Galvin-Parton PA, Erbe R, Devincentis E, Kronn D, Mofidi S, Wasserstein M, Pellegrino JE, Levy
PA, Adams DJ, Nichols M, Caggana M.
Lack of genotype-phenotype correlations and outcome in MCAD deficiency diagnosed by newborn screening in New York State.
Mol Genet Metab.
2010;99(3):263-8.
PubMed abstract
Bentler K, Zhai S, Elsbecker SA, Arnold GL, Burton BK, Vockley J, Cameron CA, Hiner SJ, Edick MJ, Berry SA.
221 newborn-screened neonates with medium-chain acyl-coenzyme A dehydrogenase deficiency: Findings from the Inborn Errors
of Metabolism Collaborative.
Mol Genet Metab.
2016;119(1-2):75-82.
PubMed abstract / Full Text
Browning MF, Levy HL, Wilkins-Haug LE, Larson C, Shih VE.
Fetal fatty acid oxidation defects and maternal liver disease in pregnancy.
Obstet Gynecol.
2006;107(1):115-20.
PubMed abstract
California Department of Health Services.
Parents' Guide to MCADD.
2005; 22. Newborn Screening Program
Carpenter K, Wiley V, Sim KG, Heath D, Wilcken B.
Evaluation of newborn screening for medium chain acyl-CoA dehydrogenase deficiency in 275 000 babies.
Arch Dis Child Fetal Neonatal Ed.
2001;85(2):F105-9.
PubMed abstract / Full Text
Chace DH, Kalas TA, Naylor EW.
The application of tandem mass spectrometry to neonatal screening for inherited disorders of intermediary metabolism.
Annu Rev Genomics Hum Genet.
2002;3:17-45.
PubMed abstract
Derks TG, Reijngoud DJ, Waterham HR, Gerver WJ, van den Berg MP, Sauer PJ, Smit GP.
The natural history of medium-chain acyl CoA dehydrogenase deficiency in the Netherlands: clinical presentation and outcome.
J Pediatr.
2006;148(5):665-670.
PubMed abstract
Feillet F, Ogier H, Cheillan D, Aquaviva C, Labarthe F, Baruteau J, Chabrol B, de Lonlay P, Valayanopoulos V, Garnotel R,
Dobbelaere D, Briand G, Jeannesson E, Vassault A, Vianey-Saban C.
[Medium-chain acyl-CoA-dehydrogenase (MCAD) deficiency: French consensus for neonatal screening, diagnosis, and management].
Arch Pediatr.
2012;19(2):184-93.
PubMed abstract
Feuchtbaum L, Carter J, Dowray S, Currier RJ, Lorey F.
Birth prevalence of disorders detectable through newborn screening by race/ethnicity.
Genet Med.
2012;14(11):937-45.
PubMed abstract
Frazier DM, Millington DS, McCandless SE, Koeberl DD, Weavil SD, Chaing SH, Muenzer J.
The tandem mass spectrometry newborn screening experience in North Carolina: 1997-2005.
J Inherit Metab Dis.
2006;29(1):76-85.
PubMed abstract
Gartner V, McGuire PJ, Lee PR.
Child Neurology: medium-chain acyl-coenzyme A dehydrogenase deficiency.
Neurology.
2015;85(4):e37-40.
PubMed abstract / Full Text
Gramer G, Haege G, Fang-Hoffmann J, Hoffmann GF, Bartram CR, Hinderhofer K, Burgard P, Lindner M.
Medium-Chain Acyl-CoA Dehydrogenase Deficiency: Evaluation of Genotype-Phenotype Correlation in Patients Detected by Newborn
Screening.
JIMD Rep.
2015;23:101-12.
PubMed abstract / Full Text
Lang TF.
Adult presentations of medium-chain acyl-CoA dehydrogenase deficiency (MCADD).
J Inherit Metab Dis.
2009;32(6):675-83.
PubMed abstract
Lee PJ, Harrison EL, Jones MG, Jones S, Leonard JV, Chalmers RA.
L-carnitine and exercise tolerance in medium-chain acyl-coenzyme A dehydrogenase (MCAD) deficiency: a pilot study.
J Inherit Metab Dis.
2005;28(2):141-52.
PubMed abstract
Leonard JV, Dezateux C.
Newborn screening for medium chain acyl CoA dehydrogenase deficiency.
Arch Dis Child.
2009;94(3):235-8.
PubMed abstract
Maier EM, Liebl B, Röschinger W, Nennstiel-Ratzel U, Fingerhut R, Olgemöller B, Busch U, Krone N, v Kries R, Roscher AA.
Population spectrum of ACADM genotypes correlated to biochemical phenotypes in newborn screening for medium-chain acyl-CoA
dehydrogenase deficiency.
Hum Mutat.
2005;25(5):443-52.
PubMed abstract
Onunaku, Ngozi.
Improving maternal and infant mental health: focus on maternal depression.
Zero to Three.
2005.
/ https://www.zerotothree.org/resource/improving-maternal-and-infant-men...
Discusses the impact of maternal depression on the social and emotional health of
young children. Recommends specific steps that early childhood programs and public health administrators can take to address
the unmet mental health needs of mothers. Ultimately promotes social and emotional health, school readiness, and the future
functioning of very young children.
Potter BK, Little J, Chakraborty P, Kronick JB, Evans J, Frei J, Sutherland SC, Wilson K, Wilson BJ.
Variability in the clinical management of fatty acid oxidation disorders: results of a survey of Canadian metabolic physicians.
J Inherit Metab Dis.
2012;35(1):115-23.
PubMed abstract
Rice GM, Steiner RD.
Inborn Errors of Metabolism (Metabolic Disorders).
Pediatr Rev.
2016;37(1):3-15; quiz 16-7, 47.
PubMed abstract
Santos L, Patterson A, Moreea SM, Lippiatt CM, Walter J, Henderson M.
Acute liver failure in pregnancy associated with maternal MCAD deficiency.
J Inherit Metab Dis.
2007;30(1):103.
PubMed abstract
Schatz UA, Ensenauer R.
The clinical manifestation of MCAD deficiency: challenges towards adulthood in the screened population.
J Inherit Metab Dis.
2010.
PubMed abstract
Tajima G, Sakura N, Yofune H, Nishimura Y, Ono H, Hasegawa Y, Hata I, Kimura M, Yamaguchi S, Shigematsu Y, Kobayashi M.
Enzymatic diagnosis of medium-chain acyl-CoA dehydrogenase deficiency by detecting 2-octenoyl-CoA production using high-performance
liquid chromatography: a practical confirmatory test for tandem mass spectrometry newborn screening in Japan.
J Chromatogr B Analyt Technol Biomed Life Sci.
2005;823(2):122-30.
PubMed abstract
Tanaka K, Gregersen N, Ribes A, Kim J, Kølvraa S, Winter V, Eiberg H, Martinez G, Deufel T, Leifert B, Santer R, François
B, Pronicka E, László A, Kmoch S, Kremensky I, Kalaydjicva L, Ozalp I, Ito M.
A survey of the newborn populations in Belgium, Germany, Poland, Czech Republic, Hungary, Bulgaria, Spain, Turkey, and Japan
for the G985 variant allele with haplotype analysis at the medium chain Acyl-CoA dehydrogenase gene locus: clinical and evolutionary
consideration.
Pediatr Res.
1997;41(2):201-9.
PubMed abstract
Therrell BL Jr, Lloyd-Puryear MA, Camp KM, Mann MY.
Inborn errors of metabolism identified via newborn screening: Ten-year incidence data and costs of nutritional interventions
for research agenda planning.
Mol Genet Metab.
2014;113(1-2):14-26.
PubMed abstract / Full Text
Waddell L, Wiley V, Carpenter K, Bennetts B, Angel L, Andresen BS, Wilcken B.
Medium-chain acyl-CoA dehydrogenase deficiency: genotype-biochemical phenotype correlations.
Mol Genet Metab.
2006;87(1):32-9.
PubMed abstract
Zytkovicz TH, Fitzgerald EF, Marsden D, Larson CA, Shih VE, Johnson DM, Strauss AW, Comeau AM, Eaton RB, Grady GF.
Tandem mass spectrometric analysis for amino, organic, and fatty acid disorders in newborn dried blood spots: a two-year summary
from the New England Newborn Screening Program.
Clin Chem.
2001;47(11):1945-55.
PubMed abstract